A Cell Profiling Framework for Modeling Drug Responses from HCS Imaging

Author:

Ng Alvin Y. J.12,Rajapakse Jagath C.12,Welsch Roy E.13,Matsudaira Paul T.14,Horodincu Victor4,Evans James G.5

Affiliation:

1. Singapore MIT Alliance, Singapore.

2. Bioinformatics Research Center, Nanyang Technological University, Singapore.

3. Sloan School of Management, MIT, Cambridge, MA.

4. Department of Biological Sciences, National University of Singapore, Singapore.

5. Anon Consulting, Cambridge, MA.

Abstract

The authors present an unsupervised, scalable, and interpretable cell profiling framework that is compatible with data gathered from high-content screening. They demonstrate the effectiveness of their framework by modeling drug differential effects of IC-21 macrophages treated with microtubule and actin disrupting drugs. They identify significant features of cell phenotypes for unsupervised learning based on maximum relevancy and minimum redundancy criteria. A 2-stage clustering approach annotates, clusters cells, and then merges them together to form super-clusters. An interpretable cell profile consisting of super-cluster proportions profiled at each drug treatment, concentration, or duration is obtained. Differential changes in super-cluster profiles are the basis for understanding the drug’s differential effect and biology. The authors’ method is validated by significant chi-squared statistics obtained from similar drug-treated super-cluster profiles from a 5-fold cross-validation. In addition, drug profiles of 2 microtubule drugs with equivalent mechanisms of action are statistically similar. Several distinct trends are identified for the 5 cytoskeletal drugs profiled under different conditions.

Publisher

Elsevier BV

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